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Abstract

In 1993, a new base, β--glucopyranosyloxymethyluracil (base J), was identified in the nuclear DNA of . Base J is the first hypermodified base found in eukaryotic DNA. It is present in all kinetoplastid flagellates analyzed and some unicellular flagellates closely related to trypanosomatids, but it has not been found in other protozoa or in metazoa. J is invariably present in the telomeric repeats of all organisms analyzed. Whereas in nearly all J is telomeric, there are other repetitive DNA sequences containing J in and , and most J is outside telomeres in . The biosynthesis of J occurs in two steps: First, a specific thymidine in DNA is converted into hydroxymethyldeoxyuridine (HOMedU), and then this HOMedU is glycosylated to form J. This review discusses the identification and localization of base J in the genome of kinetoplastids, the enzymes involved in J biosynthesis, possible biological functions of J, and J as a potential target for chemotherapy of diseases caused by kinetoplastids.

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/content/journals/10.1146/annurev.micro.62.081307.162750
2008-10-13
2024-04-18
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  • Article Type: Review Article
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